Epigenetic and genetic loss of Hic1 function accentuates the role of p53 in tumorigenesis

Wen Yong Chen; Timothy K. Cooper; Cynthia A. Zahnow; Michael Overholtzer; Zhiquan Zhao; Marc Ladanyi; Judith E. Karp; Nalan Gokgoz; Jay S. Wunder; Irene L. Andrulis; Arnold J. Levine; Joseph L. Mankowski; Stephen B. Baylin

doi:10.1016/j.ccr.2004.08.030

Epigenetic and genetic loss of Hic1 function accentuates the role of p53 in tumorigenesis

Wen Yong Chen
, Timothy K. Cooper
, Cynthia A. Zahnow
, Michael Overholtzer
, Zhiquan Zhao
, Marc Ladanyi
, Judith E. Karp
, Nalan Gokgoz
, Jay S. Wunder
, Irene L. Andrulis
, Arnold J. Levine
, Joseph L. Mankowski
, Stephen B. Baylin

Research output: Contribution to journal › Article › peer-review

141 Scopus citations

Abstract

The gene hypermethylated in cancer 1 (HIC1) is epigenetically inactivated, but not mutated, in cancer. Here we show that cooperative loss of Hic1 with p53, but not INK4a, yields distinct tumor phenotypes in mice. Germline deletion of one allele of each gene on the opposite chromosome yields breast and ovarian carcinomas and metastatic osteosarcomas with epigenetic inactivation of the wild-type Hic1 allele. Germline deletion of the two genes on the same chromosome results in earlier appearance and increased prevalence and aggressiveness of osteosarcomas with genetic deletion of both wild-type genes. In human osteosarcomas, hypermethylation of HIC1 is frequent only in tumors with p53 mutations. Our results indicate the importance of genes altered only through epigenetic mechanisms in cancer progression in conjunction with genetically modified tumor suppressor genes.

Original language	English (US)
Pages (from-to)	387-398
Number of pages	12
Journal	Cancer Cell
Volume	6
Issue number	4
DOIs	https://doi.org/10.1016/j.ccr.2004.08.030
State	Published - Oct 2004

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

All Science Journal Classification (ASJC) codes

Oncology
Cell Biology
Cancer Research

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10.1016/j.ccr.2004.08.030

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@article{316d186102f34a959ab5fc6493292a1b,

title = "Epigenetic and genetic loss of Hic1 function accentuates the role of p53 in tumorigenesis",

abstract = "The gene hypermethylated in cancer 1 (HIC1) is epigenetically inactivated, but not mutated, in cancer. Here we show that cooperative loss of Hic1 with p53, but not INK4a, yields distinct tumor phenotypes in mice. Germline deletion of one allele of each gene on the opposite chromosome yields breast and ovarian carcinomas and metastatic osteosarcomas with epigenetic inactivation of the wild-type Hic1 allele. Germline deletion of the two genes on the same chromosome results in earlier appearance and increased prevalence and aggressiveness of osteosarcomas with genetic deletion of both wild-type genes. In human osteosarcomas, hypermethylation of HIC1 is frequent only in tumors with p53 mutations. Our results indicate the importance of genes altered only through epigenetic mechanisms in cancer progression in conjunction with genetically modified tumor suppressor genes.",

author = "Chen, \{Wen Yong\} and Cooper, \{Timothy K.\} and Zahnow, \{Cynthia A.\} and Michael Overholtzer and Zhiquan Zhao and Marc Ladanyi and Karp, \{Judith E.\} and Nalan Gokgoz and Wunder, \{Jay S.\} and Andrulis, \{Irene L.\} and Levine, \{Arnold J.\} and Mankowski, \{Joseph L.\} and Baylin, \{Stephen B.\}",

note = "Funding Information: We thank B. Davis for assistance with ovarian tumor classification, K. Jair, D. Otteson, S. Sabunciyan, K. Schuebel, and S. Sharkis for critical reading of the manuscript, P. Wilcox and JHU Reference Histology Lab for assistance in histology, and L. Meszler for assistance of microscopy. This study was supported by a grant from the US National Institute of Health to S.B.B.",

year = "2004",

month = oct,

doi = "10.1016/j.ccr.2004.08.030",

language = "English (US)",

volume = "6",

pages = "387--398",

journal = "Cancer Cell",

issn = "1535-6108",

publisher = "Cell Press",

number = "4",

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T1 - Epigenetic and genetic loss of Hic1 function accentuates the role of p53 in tumorigenesis

AU - Chen, Wen Yong

AU - Cooper, Timothy K.

AU - Zahnow, Cynthia A.

AU - Overholtzer, Michael

AU - Zhao, Zhiquan

AU - Ladanyi, Marc

AU - Karp, Judith E.

AU - Gokgoz, Nalan

AU - Wunder, Jay S.

AU - Andrulis, Irene L.

AU - Levine, Arnold J.

AU - Mankowski, Joseph L.

AU - Baylin, Stephen B.

N1 - Funding Information: We thank B. Davis for assistance with ovarian tumor classification, K. Jair, D. Otteson, S. Sabunciyan, K. Schuebel, and S. Sharkis for critical reading of the manuscript, P. Wilcox and JHU Reference Histology Lab for assistance in histology, and L. Meszler for assistance of microscopy. This study was supported by a grant from the US National Institute of Health to S.B.B.

PY - 2004/10

Y1 - 2004/10

N2 - The gene hypermethylated in cancer 1 (HIC1) is epigenetically inactivated, but not mutated, in cancer. Here we show that cooperative loss of Hic1 with p53, but not INK4a, yields distinct tumor phenotypes in mice. Germline deletion of one allele of each gene on the opposite chromosome yields breast and ovarian carcinomas and metastatic osteosarcomas with epigenetic inactivation of the wild-type Hic1 allele. Germline deletion of the two genes on the same chromosome results in earlier appearance and increased prevalence and aggressiveness of osteosarcomas with genetic deletion of both wild-type genes. In human osteosarcomas, hypermethylation of HIC1 is frequent only in tumors with p53 mutations. Our results indicate the importance of genes altered only through epigenetic mechanisms in cancer progression in conjunction with genetically modified tumor suppressor genes.

AB - The gene hypermethylated in cancer 1 (HIC1) is epigenetically inactivated, but not mutated, in cancer. Here we show that cooperative loss of Hic1 with p53, but not INK4a, yields distinct tumor phenotypes in mice. Germline deletion of one allele of each gene on the opposite chromosome yields breast and ovarian carcinomas and metastatic osteosarcomas with epigenetic inactivation of the wild-type Hic1 allele. Germline deletion of the two genes on the same chromosome results in earlier appearance and increased prevalence and aggressiveness of osteosarcomas with genetic deletion of both wild-type genes. In human osteosarcomas, hypermethylation of HIC1 is frequent only in tumors with p53 mutations. Our results indicate the importance of genes altered only through epigenetic mechanisms in cancer progression in conjunction with genetically modified tumor suppressor genes.

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UR - https://www.scopus.com/pages/publications/5444259434#tab=citedBy

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DO - 10.1016/j.ccr.2004.08.030

M3 - Article

C2 - 15488761

AN - SCOPUS:5444259434

SN - 1535-6108

VL - 6

SP - 387

EP - 398

JO - Cancer Cell

JF - Cancer Cell

IS - 4

ER -

Epigenetic and genetic loss of Hic1 function accentuates the role of p53 in tumorigenesis

Abstract

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